Literature DB >> 20849117

Superadditive effects of ethanol and flunitrazepam: implications of using immunopharmacotherapy as a therapeutic.

Jennifer B Treweek1, Amanda J Roberts, Kim D Janda.   

Abstract

While benzodiazepine intoxication alone may elicit sedative and antianxiety effects, alcohol coingestion greatly amplifies this central nervous system depression. As a result, this drug combination gained notoriety for its role in cases of facilitated sexual assault and fatal overdose. We previously validated the ability of the novel antiflunitrazepam monoclonal antibody (mAb) RCA3A3 to bind flunitrazepam (FLU) in vivo and block FLU-induced impairment of locomotion and memory. A therapeutically relevant application of this high affinity mAb (K(d,app) = 200 nM), however, is to the more tenuous indication of flunitrazepam (FLU) and alcohol cointoxication. Employing a murine behavioral model, passive immunization with mAb RCA3A3 before injection of ethanol (EtOH: low-dose, 1 g/kg, or high-dose, 1.5 g/kg), FLU (0.06 mg/kg), or a cocktail of both drugs offered partial to full restoration of motor activity levels in co-drug treated and FLU-treated mouse groups (n = 12), respectively. Whereas all drug treatments left contextual learning intact, auditory cued learning was severely disrupted. Prophylactic administration of mAb RCA3A3 prevented this deficit in cued learning in FLU-treated mice but not in the FLU- and EtOH-treated mice, in which co-drug exposure exacerbated the impairment in cued fear conditioning. To substantiate this finding, a dose-response study was performed, and the changes in locomotor activity incurred by different FLU (low-dose, 0.06 mg/kg, or high-dose, 0.09 mg/kg), EtOH (1.0 g/kg, 1.5 g/kg), and mAb RCA3A3 (14.5 mg/kg, 21.8 mg/kg) dose combinations illustrated the potentiation in motor effects by concomitant exposure to FLU and EtOH. Thus, motor activity and fear conditioning results demonstrated that both the amount of FLU left unbound by antibody and the pharmacological additivity between FLU and EtOH, a GABA mimetic, were limiting factors in the therapeutic efficacy of mAb RCA3A3. In sum, our study highlights the complex nature of psychomotor impairment upon co-drug versus singular drug exposure, which may pose a unique challenge to therapeutic treatment.

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Year:  2010        PMID: 20849117      PMCID: PMC2997924          DOI: 10.1021/mp900293a

Source DB:  PubMed          Journal:  Mol Pharm        ISSN: 1543-8384            Impact factor:   4.939


  38 in total

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4.  Contextual fear conditioning and baseline startle responses in the rat fear-potentiated startle test: a comparison of benzodiazepine/gamma-aminobutyric acid-A receptor agonists.

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5.  Contextual control over the expression of fear in rats conditioned under a benzodiazepine.

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7.  Relative potency and effectiveness of flunitrazepam, ethanol, and beta-CCE for disrupting the acquisition and retention of response sequences in rats.

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8.  Passive immunization with a nicotine-specific monoclonal antibody decreases brain nicotine levels but does not precipitate withdrawal in nicotine-dependent rats.

Authors:  Samuel A Roiko; Andrew C Harris; Mark G LeSage; Daniel E Keyler; Paul R Pentel
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9.  Prevention of drug-induced memory impairment by immunopharmacotherapy.

Authors:  Jennifer B Treweek; Chengzao Sun; Alexander V Mayorov; Longwu Qi; Coree L Levy; Amanda J Roberts; Tobin J Dickerson; Kim D Janda
Journal:  J Med Chem       Date:  2008-10-16       Impact factor: 7.446

10.  Effects of ethanol on encoding, consolidation, and expression of extinction following contextual fear conditioning.

Authors:  K Matthew Lattal
Journal:  Behav Neurosci       Date:  2007-12       Impact factor: 1.912

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3.  Effect of flunitrazepam as an oral hypnotic on 24-hour blood pressure in healthy volunteers.

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